Tracking sub-clonal <i>TP53</i> mutated tumor cells in human metastatic renal cell carcinoma

Bousquet, Guilhem; Bouchtaoui, Morad El; Lebœuf, Christophe; Battistella, Maxime; Varna, Mariana; Ferreira, I.; Plassa, Louis-François; Hamdan, Diaddin; Bertheau, Philippe; Feugeas, Jean-Paul; Damotte, Diane; Janin, Anne

doi:10.18632/oncotarget.4220

Cited by 28 publications

(28 citation statements)

References 24 publications

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“…Because TP53 is ubiquitously altered in cancers, TP53 mutations are a tool to confirm the provenance of PDTX (Park et al 2013;Walters et al 2013;Dodbiba et al 2015). Moreover, selection pressures that lead to expansion of aggressive clones on implantation of primary tumors appear to replicate metastatic colonization such that TP53 mutations found in PTDX can serve as a beacon to track the origin of metastases back to minor subclones present in the primary tumors (Bousquet et al 2015). Additional resources and further development are needed before PTDX can become an integral part of a cancer patient's clinical care as a platform to help define therapies based on the molecular make-up of an individual tumor.…”

Section: Tp53 At the Crossroads Of Clinical Genomics And Cancer Therapymentioning

confidence: 99%

Clinical Outcomes of TP53 Mutations in Cancers

Robles

Jen

Harris

2016

Cold Spring Harb Perspect Med

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High-throughput sequencing of cancer genomes is increasingly becoming an essential tool of clinical oncology that facilitates target identification and targeted therapy within the context of precision medicine. The cumulative profiles of somatic mutations in cancer yielded by comprehensive molecular studies also constitute a fingerprint of historical exposures to exogenous and endogenous mutagens, providing insight into cancer evolution and etiology. Mutational signatures that were first established by inspection of the TP53 gene somatic landscape have now been confirmed and expanded by comprehensive sequencing studies. Further, the degree of granularity achieved by deep sequencing allows detection of low-abundance mutations with clinical relevance. In tumors, they represent the emergence of small aggressive clones; in normal tissues, they signal a mutagenic exposure related to cancer risk; and, in blood, they may soon become effective surveillance tools for diagnostic purposes and for monitoring of cancer prognosis and recurrence.

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Section: Tp53 At the Crossroads Of Clinical Genomics And Cancer Therapymentioning

confidence: 99%

Clinical Outcomes of TP53 Mutations in Cancers

Robles

Jen

Harris

2016

Cold Spring Harb Perspect Med

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“…One major limitation is the low engraftment rate of patient-derived xenografts, usually under 20% for localized primary tumors grafted subcutaneously [28,31,33,49]. Certain experimental conditions may significantly increase this rate: orthotopic grafting, grafting under the renal capsule [35,50], or estradiol supplementation for breast cancer xenografts [35].…”

Section: What Could Limit Their Use For Preclinical Development Of Anmentioning

confidence: 99%

“…We established xenograft models of human primary RCCs, with an engraftment rate of 5% in case of localized disease, and of 36% in case of metastatic disease at diagnosis [31,49]. For each xenograft model, we compared the primary tumor and the corresponding tumor xenografts at the first passage.…”

Section: Could Patient-derived Xenografts Reflect Metastatic Disease?mentioning

confidence: 99%

Patient-Derived Xenograft: An Adjuvant Technology for the Treatment of Metastatic Disease

Bousquet

Janin²

2016

Pathobiology

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The occurrence of metastases severely affects prognosis for patients with cancer, making metastatic disease a daily societal challenge. Because of resistance to drugs, the potential curability with chemotherapy at the metastatic stage remains low. Large genomic analyses to identify new targets have their limitations due to intratumor heterogeneity when they are performed on tumor samples from primary tumors and because the functional value of molecular abnormalities in a cancer is usually not known. Additional tools are thus required for the development of new anticancer agents. The use of preclinical models is a key component of translational research in oncology. For four decades, xenograft models of human cancer cell lines injected subcutaneously in immunocompromised mice have been widely used, with disappointing results for predicting the clinical benefit of a new drug. Patient-derived xenografts are preclinical models rediscovered as innovative pharmacological tools, both for the preclinical development of anticancer drugs and as individual models for personalized treatment of metastatic disease. Here, we review the recent progress reported using patient-derived xenografts for the treatment of metastatic disease, and discuss the feasibility of their implementation in daily oncological care.

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“…Dans ces modèles, une stabilité histologique et moléculaire par rapport à la tumeur d'origine peut être observée [45] et la stabilité vis-à-vis de la réponse aux traitements antiangiogéniques est également retrouvée. Cependant, la souris athymique ne présentant pas de lymphocytes cytotoxiques (LT8, lymphocytes T CD8 + ), il est important de relier ces résultats à la nature du tissu d'origine et aux données cliniques, et d'évaluer, dans les tissus, l'infiltration des LT8 et l'expression de PDL-1 (programmed deathligand 1), inhibiteur des LT8, qui peut varier selon le type de tumeur [46].…”

Section: Référencesunclassified

“…La microdissection de cellules endothéliales réalisée à partir de biopsies de métastases, confirme ces observations [24]. Nous avons montré que les modèles expérimentaux précliniques que nous avons développés sont pertinents car la plupart des tumeurs aptes à se développer dans la souris athymique sont les clones les plus agressifs [23,24,45,49]. La possibilité d'identifier différents marqueurs, notamment au niveau des niches de précurseurs endothé-liaux, ouvre une voie nouvelle dans la prise en charge des traitements antiangiogéniques.…”

Section: Référencesunclassified